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rate data fitting software originpro 8.5 (OriginLab corp)

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OriginLab corp rate data fitting software originpro 8.5
Rate Data Fitting Software Originpro 8.5, supplied by OriginLab corp, used in various techniques. Bioz Stars score: 90/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/rate data fitting software originpro 8.5/product/OriginLab corp
Average 90 stars, based on 1 article reviews

rate data fitting software originpro 8.5 - by Bioz Stars, 2026-06

90/100 stars

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Comparison of the pvT data measured with the HCR and the 2-Domain Tait model fitted based on HCR data and those provided by <t>Moldflow.</t>

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data fitting software origin(pro) version 2016 (OriginLab corp)

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$a Simplified representation of the 70S ribosome with the AMK binding site indicated with the blue star. b The unbiased ( F o – F c ) difference electron density map of AMK bound near the decoding center is contoured at 2.3σ. c AMK binds within helix h44 of the decoding center where the AHB moiety forms three unique interactions. d Time courses of f[ 3 H]Met-Phe-Phe tripeptide formation with EF-Tu ternary complex (TC) (5 μM) and EF-G (5 µM) in the absence (black) and presence of 20 μM AMK (red). Solid lines represent the double exponential fit of the data with SEM from n = 3 independent experiments. e Time evolution of fluorescence traces obtained for the EF-G (5 μM) catalyzed movement of pyrene-labeled mRNA on 70S ribosomes (0.5 μM) in the presence of various concentrations (0-5 µM) of AMK. The inhibition of mRNA movement by AMK was estimated from amplitudes of the slow phase of fluorescence traces relative to the total transition (normalized to 1) indicative of inhibited fraction of the ribosomes. f The fraction of AMK-inhibited pre-TC plotted against AMK concentration. Data were fitted with hyperbolic function (solid line) and half-inhibitory concentration ( K I ) of AMK on the inhibition of translocation was estimated from mid-point of transition. Experiments were conducted in <t>triplicates</t> and error bars indicate the SEM of data.$
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Image Search Results

Comparison of the pvT data measured with the HCR and the 2-Domain Tait model fitted based on HCR data and those provided by Moldflow.

Journal: Polymers

Article Title: Analysis of the Similarity between Injection Molding Simulation and Experiment

doi: 10.3390/polym16091265

Figure Lengend Snippet: Comparison of the pvT data measured with the HCR and the 2-Domain Tait model fitted based on HCR data and those provided by Moldflow.

Article Snippet: The measurement data were subsequently used to model the Cross-WLF model [ ] using Autodesk Moldflow Data Fitting Software [ ].

Techniques: Comparison

Comparison of the viscosities measured with the HCR and the Cross-WLF models fitted based on the HCR data and those provided by Moldflow.

Journal: Polymers

Article Title: Analysis of the Similarity between Injection Molding Simulation and Experiment

doi: 10.3390/polym16091265

Figure Lengend Snippet: Comparison of the viscosities measured with the HCR and the Cross-WLF models fitted based on the HCR data and those provided by Moldflow.

Article Snippet: The measurement data were subsequently used to model the Cross-WLF model [ ] using Autodesk Moldflow Data Fitting Software [ ].

Techniques: Comparison

Comparison of the thermal conductivity measured and those provided by Moldflow.

Journal: Polymers

Article Title: Analysis of the Similarity between Injection Molding Simulation and Experiment

doi: 10.3390/polym16091265

Figure Lengend Snippet: Comparison of the thermal conductivity measured and those provided by Moldflow.

Article Snippet: The measurement data were subsequently used to model the Cross-WLF model [ ] using Autodesk Moldflow Data Fitting Software [ ].

Techniques: Comparison

Comparison of the time series of the flow rate, cavity pressure and injection pressure measured in the experiment with the time series calculated in the simulation using the material data card from Moldflow and the material data fitted.

Journal: Polymers

Article Title: Analysis of the Similarity between Injection Molding Simulation and Experiment

doi: 10.3390/polym16091265

Figure Lengend Snippet: Comparison of the time series of the flow rate, cavity pressure and injection pressure measured in the experiment with the time series calculated in the simulation using the material data card from Moldflow and the material data fitted.

Article Snippet: The measurement data were subsequently used to model the Cross-WLF model [ ] using Autodesk Moldflow Data Fitting Software [ ].

Techniques: Comparison, Injection

$a Simplified representation of the 70S ribosome with the AMK binding site indicated with the blue star. b The unbiased ( F o – F c ) difference electron density map of AMK bound near the decoding center is contoured at 2.3σ. c AMK binds within helix h44 of the decoding center where the AHB moiety forms three unique interactions. d Time courses of f[ 3 H]Met-Phe-Phe tripeptide formation with EF-Tu ternary complex (TC) (5 μM) and EF-G (5 µM) in the absence (black) and presence of 20 μM AMK (red). Solid lines represent the double exponential fit of the data with SEM from n = 3 independent experiments. e Time evolution of fluorescence traces obtained for the EF-G (5 μM) catalyzed movement of pyrene-labeled mRNA on 70S ribosomes (0.5 μM) in the presence of various concentrations (0-5 µM) of AMK. The inhibition of mRNA movement by AMK was estimated from amplitudes of the slow phase of fluorescence traces relative to the total transition (normalized to 1) indicative of inhibited fraction of the ribosomes. f The fraction of AMK-inhibited pre-TC plotted against AMK concentration. Data were fitted with hyperbolic function (solid line) and half-inhibitory concentration ( K I ) of AMK on the inhibition of translocation was estimated from mid-point of transition. Experiments were conducted in triplicates and error bars indicate the SEM of data.$

Journal: Nature Communications

Article Title: Molecular basis of the pleiotropic effects by the antibiotic amikacin on the ribosome

doi: 10.1038/s41467-023-40416-5

Figure Lengend Snippet: a Simplified representation of the 70S ribosome with the AMK binding site indicated with the blue star. b The unbiased ( F o – F c ) difference electron density map of AMK bound near the decoding center is contoured at 2.3σ. c AMK binds within helix h44 of the decoding center where the AHB moiety forms three unique interactions. d Time courses of f[ 3 H]Met-Phe-Phe tripeptide formation with EF-Tu ternary complex (TC) (5 μM) and EF-G (5 µM) in the absence (black) and presence of 20 μM AMK (red). Solid lines represent the double exponential fit of the data with SEM from n = 3 independent experiments. e Time evolution of fluorescence traces obtained for the EF-G (5 μM) catalyzed movement of pyrene-labeled mRNA on 70S ribosomes (0.5 μM) in the presence of various concentrations (0-5 µM) of AMK. The inhibition of mRNA movement by AMK was estimated from amplitudes of the slow phase of fluorescence traces relative to the total transition (normalized to 1) indicative of inhibited fraction of the ribosomes. f The fraction of AMK-inhibited pre-TC plotted against AMK concentration. Data were fitted with hyperbolic function (solid line) and half-inhibitory concentration ( K I ) of AMK on the inhibition of translocation was estimated from mid-point of transition. Experiments were conducted in triplicates and error bars indicate the SEM of data.

Article Snippet: Experiments were conducted in triplicates, data were fitted in Origin(Pro), Version 2016 (OriginLab Corp.), and error bars indicate the SEM of data.

Techniques: Binding Assay, Fluorescence, Labeling, Inhibition, Concentration Assay, Translocation Assay

$a Time courses of BOP-Met-Phe-Leu release from the P site of the ribosomes in pre-TC (0.1 μM) upon mixing with RF2 (1 μM) in the presence of various concentrations of AMK (0-1 μM). The near monophasic curves are fitted with double exponential function (solid lines) and the rates and amplitudes of the predominant fast phase (> 99%) were determined. The fraction inhibited was estimated from the fractional loss in fluorescence amplitude for a given AMK concentration considering the total amplitude of fluorescence transition (without AMK) as 1. b Fraction inhibition of RF2-mediated peptide release as the function of increasing concentrations of AMK. Solid line is the hyperbolic fit of data from which half-maximal inhibitory concentration ( K I ) of AMK for peptide release was estimated. c Time tra c es for Rayleigh light scattering upon splitting of post-TC ribosomes (0.5 μM) into subunits by the concerted action of RRF (20 μM) and EF-G (10 μM) in the presence of various concentrations of AMK (0–20 μM). The scattering traces were fitted with double exponential function and the rates and amplitudes of both the fast and slow phases were determined. d Fraction inhibition of RRF and EF-G-mediated ribosome splitting was estimated from the fractional loss of the amplitude of the fast phase considering amplitude of the entire transition without AMK as 1. The solid line represents the hyperbolic fit of the fraction inhibition plotted against AMK concentration from which the half-maximal concentration ( K I ) of AMK to inhibit ribosome recycling was estimated. Experiments were conducted in triplicates, data were fitted in Origin(Pro), Version 2016 (OriginLab Corp.), and error bars indicate the SEM of data.$

Journal: Nature Communications

Article Title: Molecular basis of the pleiotropic effects by the antibiotic amikacin on the ribosome

doi: 10.1038/s41467-023-40416-5

Figure Lengend Snippet: a Time courses of BOP-Met-Phe-Leu release from the P site of the ribosomes in pre-TC (0.1 μM) upon mixing with RF2 (1 μM) in the presence of various concentrations of AMK (0-1 μM). The near monophasic curves are fitted with double exponential function (solid lines) and the rates and amplitudes of the predominant fast phase (> 99%) were determined. The fraction inhibited was estimated from the fractional loss in fluorescence amplitude for a given AMK concentration considering the total amplitude of fluorescence transition (without AMK) as 1. b Fraction inhibition of RF2-mediated peptide release as the function of increasing concentrations of AMK. Solid line is the hyperbolic fit of data from which half-maximal inhibitory concentration ( K I ) of AMK for peptide release was estimated. c Time tra c es for Rayleigh light scattering upon splitting of post-TC ribosomes (0.5 μM) into subunits by the concerted action of RRF (20 μM) and EF-G (10 μM) in the presence of various concentrations of AMK (0–20 μM). The scattering traces were fitted with double exponential function and the rates and amplitudes of both the fast and slow phases were determined. d Fraction inhibition of RRF and EF-G-mediated ribosome splitting was estimated from the fractional loss of the amplitude of the fast phase considering amplitude of the entire transition without AMK as 1. The solid line represents the hyperbolic fit of the fraction inhibition plotted against AMK concentration from which the half-maximal concentration ( K I ) of AMK to inhibit ribosome recycling was estimated. Experiments were conducted in triplicates, data were fitted in Origin(Pro), Version 2016 (OriginLab Corp.), and error bars indicate the SEM of data.

Article Snippet: Experiments were conducted in triplicates, data were fitted in Origin(Pro), Version 2016 (OriginLab Corp.), and error bars indicate the SEM of data.

Techniques: Fluorescence, Concentration Assay, Inhibition